ErbB signaling in cardiac development and disease

Sanchez-Soria, Pablo; Camenisch, Todd D.

doi:10.1016/j.semcdb.2010.09.011

Cited by 67 publications

(52 citation statements)

References 95 publications

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“…Nfatc1 is required downstream from VEGF to regulate the extent of EMT and sustain endocardial proliferation during EMT and post-EMT valve elongation (Chang et al 2004;Wu et al 2011;Lin et al 2012). The ErbB/SHP-2/NF-1/Ras signaling axis promotes mesenchymal migration into the cardiac jelly and proliferation and expansion of cushion mesenchyme Iwamoto and Mekada 2006;Sanchez-Soria and Camenisch 2010).…”

Section: Patterning Of Cardiac Valve Territory and Emtmentioning

confidence: 99%

How to Make a Heart Valve: From Embryonic Development to Bioengineering of Living Valve Substitutes

MacGrogan

Luxán

Driessen-Mol

et al. 2014

Cold Spring Harbor Perspectives in Medicine

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Section: Patterning Of Cardiac Valve Territory and Emtmentioning

confidence: 99%

How to Make a Heart Valve: From Embryonic Development to Bioengineering of Living Valve Substitutes

MacGrogan

Luxán

Driessen-Mol

et al. 2014

Cold Spring Harbor Perspectives in Medicine

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“…A feature that enables the HER family of receptors to control diverse signaling outputs is their ability to utilize their phosphorylation sites in a combinatorial manner through receptor heterodimerization. The combined outputs from specific pairs of HER family members are important for many fundamental biological processes, including heart function ( 2, 3 ), the proliferation of Schwann cells ( 4 ), and neurogenesis ( 5 ).…”

Section: Introductionmentioning

confidence: 99%

Structural analysis of the EGFR/HER3 heterodimer reveals the molecular basis for activating HER3 mutations

et al. 2014

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The human epidermal growth factor receptor (HER) tyrosine kinases homo- and hetero-dimerize to activate downstream signaling pathways. HER3 is a catalytically impaired member of the HER family that contributes to the development of several human malignancies and is mutated in a subset of cancers. HER3 signaling depends on heterodimerization with a catalytically active partner, in particular EGFR (the founding family member, also known as HER1) or HER2. The activity of homodimeric complexes of catalytically active HER family members depends on allosteric activation between the two kinase domains. To determine the structural basis for HER3 signaling through heterodimerization with a catalytically active HER receptor, we solved the crystal structure of the heterodimeric complex formed by the isolated kinase domains of EGFR and HER3. The structure visualized HER3 as an allosteric activator of EGFR and revealed a conserved role of the allosteric mechanism in activation of HER family members through heterodimerization. To understand the effects of cancer-associated HER3 mutations at the molecular level, we solved the structures of two HER3 kinase mutants, each in a heterodimeric complex with the kinase domain of EGFR. These structures, combined with biochemical analysis and molecular dynamics simulations, indicated that the cancer-associated HER3 mutations enhanced the allosteric potential of HER3 by redesigning local interactions at the dimerization interface.

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“…gene regulation | patterning | follicle cells E pidermal growth factor receptor (EGFR) controls multiple developmental processes, including body axes specification in insects (1), vulval patterning in nematodes (2), skin pigmentation in fish (3), and cardiac development in humans (4). Drosophila oogenesis is one of the most extensively studied models of EGFR signaling in development.…”

mentioning

confidence: 99%

Transcriptional interpretation of the EGF receptor signaling gradient

Fuchs

Cheung

Charbonnier

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Epidermal growth factor receptor (EGFR) controls a wide range of developmental events, from body axes specification in insects to cardiac development in humans. During Drosophila oogenesis, a gradient of EGFR activation patterns the follicular epithelium. Multiple transcriptional targets of EGFR in this tissue have been identified, but their regulatory elements are essentially unknown. We report the regulatory elements of broad ( br ) and pipe ( pip ), two important targets of EGFR signaling in Drosophila oogenesis. br is expressed in a complex pattern that prefigures the formation of respiratory eggshell appendages. We found that this pattern is generated by dynamic activities of two regulatory elements, which display different responses to Pointed, Capicua, and Mirror, transcription factors involved in the EGFR-mediated gene expression. One of these elements is active in a pattern similar to pip , a gene repressed by EGFR and essential for establishing the dorsoventral polarity of the embryo. We demonstrate that this similarity of expression depends on a common sequence motif that binds Mirror in vitro and is essential for transcriptional repression in vivo.

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ErbB signaling in cardiac development and disease

Cited by 67 publications

References 95 publications

How to Make a Heart Valve: From Embryonic Development to Bioengineering of Living Valve Substitutes

How to Make a Heart Valve: From Embryonic Development to Bioengineering of Living Valve Substitutes

Structural analysis of the EGFR/HER3 heterodimer reveals the molecular basis for activating HER3 mutations

Transcriptional interpretation of the EGF receptor signaling gradient

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